Takeo Yukari H, Kakegawa Wataru, Miura Eriko, Yuzaki Michisuke
Department of Physiology, Keio University School of Medicine, Tokyo 160-8582, Japan, and Core Research for Evolutional Science and Technology (CREST), Japan Science and Technology Agency (JST), Tokyo 102-0075, Japan.
Department of Physiology, Keio University School of Medicine, Tokyo 160-8582, Japan, and Core Research for Evolutional Science and Technology (CREST), Japan Science and Technology Agency (JST), Tokyo 102-0075, Japan
J Neurosci. 2015 Sep 9;35(36):12518-34. doi: 10.1523/JNEUROSCI.0075-15.2015.
The establishment of cell-type-specific dendritic arbors is fundamental for proper neural circuit formation. Here, using temporal- and cell-specific knock-down, knock-out, and overexpression approaches, we show that multiple aspects of the dendritic organization of cerebellar Purkinje cells (PCs) are controlled by a single transcriptional factor, retinoic acid-related orphan receptor-alpha (RORα), a gene defective in staggerer mutant mice. As reported earlier, RORα was required for regression of primitive dendrites before postnatal day 4 (P4). RORα was also necessary for PCs to form a single Purkinje layer from P0 to P4. The knock-down of RORα from P4 impaired the elimination of perisomatic dendrites and maturation of single stem dendrites in PCs at P8. Filopodia and spines were also absent in these PCs. The knock-down of RORα from P8 impaired the formation and maintenance of terminal dendritic branches of PCs at P14. Finally, even after dendrite formation was completed at P21, RORα was required for PCs to maintain dendritic complexity and functional synapses, but their mature innervation pattern by single climbing fibers was unaffected. Interestingly, overexpression of RORα in PCs at various developmental stages did not facilitate dendrite development, but had specific detrimental effects on PCs. Because RORα deficiency during development is closely related to the severity of spinocerebellar ataxia type 1, delineating the specific roles of RORα in PCs in vivo at different time windows during development and throughout adulthood would facilitate our understanding of the pathogenesis of cerebellar disorders. Significance statement: The genetic programs by which each neuron subtype develops and maintains dendritic arbors have remained largely unclear. This is partly because dendrite development is modulated dynamically by neuronal activities and interactions with local environmental cues in vivo. In addition, dendrites are formed and maintained by the balance between their growth and regression; the effects caused by the disruption of transcription factors during the early developmental stages could be masked by dendritic growth or regression in the later stages. Here, using temporal- and cell-specific knock-down, knock-out, and overexpression approaches in vivo, we show that multiple aspects of the dendritic organization of cerebellar Purkinje cells are controlled by a single transcriptional factor, retinoic acid-related orphan receptor alpha.
细胞类型特异性树突分支的建立对于正确的神经回路形成至关重要。在此,我们使用时间和细胞特异性的敲低、敲除和过表达方法,表明小脑浦肯野细胞(PCs)树突组织的多个方面受单一转录因子维甲酸相关孤儿受体α(RORα)的控制,该基因在蹒跚突变小鼠中存在缺陷。如先前报道,RORα是出生后第4天(P4)前原始树突退化所必需的。RORα对于PCs在P0到P4形成单个浦肯野层也是必需的。从P4开始敲低RORα会损害P8时PCs中胞体周围树突的消除和单个主干树突的成熟。这些PCs中也不存在丝状伪足和棘突。从P8开始敲低RORα会损害P14时PCs终末树突分支的形成和维持。最后,即使在P21树突形成完成后,PCs维持树突复杂性和功能性突触仍需要RORα,但它们由单根攀缘纤维形成的成熟支配模式不受影响。有趣的是,在不同发育阶段PCs中过表达RORα并不会促进树突发育,反而对PCs有特定的有害影响。由于发育过程中RORα的缺乏与1型脊髓小脑共济失调的严重程度密切相关,阐明RORα在发育过程中不同时间窗口以及整个成年期PCs体内的特定作用将有助于我们理解小脑疾病的发病机制。意义声明:每种神经元亚型发育和维持树突分支的遗传程序在很大程度上仍不清楚。部分原因是树突发育在体内受神经元活动和与局部环境线索相互作用的动态调节。此外,树突通过其生长和退化之间的平衡形成和维持;早期发育阶段转录因子破坏所导致的影响可能会被后期树突的生长或退化所掩盖。在此,我们在体内使用时间和细胞特异性的敲低、敲除和过表达方法,表明小脑浦肯野细胞树突组织的多个方面受单一转录因子维甲酸相关孤儿受体α的控制。